视网膜色素上皮细胞系吞噬溶酶体活化的抑制。

A W Taylor, S Dixit, J Yu
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摘要

眼睛是一种具有多种免疫抑制机制的免疫特权组织,以保护聚光组织免受炎症的损害。其中一种机制涉及视网膜色素上皮细胞对巨噬细胞吞噬体激活的抑制。这项工作的目的是确定人RPE细胞系ARPE-19是否能够以类似于原代RPE的方式抑制巨噬细胞中吞噬酶体的激活。制备人ARPE-19细胞的条件培养基、亚融合培养、仅融合培养和已建立的融合培养。这些条件培养基用于巨噬细胞吞噬pHrodo生物颗粒。孵育24小时后,用荧光显微镜对巨噬细胞成像,并测量荧光。荧光强度与被吞噬的生物颗粒的数量成正比,并处于活化的吞噬溶酶体中。小鼠原位RPE眼杯条件培养基显著抑制吞噬酶体的激活。人ARPE-19细胞培养的条件培养基,培养到亚融合(50%)或培养到融合,对吞噬酶体的激活没有影响。相比之下,来自已建立的融合培养的条件培养基显著抑制吞噬酶体的激活。从已建立的融合ARPE-19细胞培养的条件培养基中去除神经肽α - msh和NPY。这种耗尽的条件培养基减少了对吞噬酶体激活的抑制,同时促进了巨噬细胞的死亡。此外,从割伤的ARPE-19单层培养物中提取的条件培养基对吞噬酶体激活的抑制作用减弱。本技术报告提示,与原代RPE单层细胞一样,建立的ARPE-19细胞融合培养也能产生抑制巨噬细胞活化的可溶性因子,可用于研究视网膜免疫生物学的分子机制。此外,结果进一步证明了完整的RPE细胞单层对调节眼内免疫细胞活性的重要性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Retinal Pigment Epithelial Cell Line Suppression of Phagolysosome Activation.

The eye is an immune privileged tissue with multiple mechanisms of immunosuppression to protect the light gathering tissues from the damage of inflammation. One of theses mechanisms involves retinal pigment epithelial cell suppression of phagosome activation in macrophages. The objective of this work is to determine if the human RPE cell line ARPE-19 is capable of suppressing the activation of the phagolysosome in macrophages in a manner similar to primary RPE. The conditioned media of RPE eyecups, sub-confluent, just confluent cultures, or established confluent cultures of human ARPE-19 cells were generated. These condition media were used to treat macrophages phagocytizing pHrodo bioparticles. After 24 hours incubation the macrophages were imaged by fluorescent microscopy, and fluorescence was measured. The fluorescent intensity is proportional to the amount of bioparticles phagocytized and are in an activated phagolysosome. The conditioned media of in situ mouse RPE eyecups significantly suppressed the activation of phagolysosome. The conditioned media from cultures of human ARPE-19 cells, grown to sub-confluence (50%) or grown to confluence had no effect on phagolysosome activation. In contrast, the conditioned media from established confluent cultures significantly suppressed phagolysosome activation. The neuropeptides alpha-MSH and NPY were depleted from the conditioned media of established confluent ARPE-19 cell cultures. This depleted conditioned media had diminished suppression of phagolysosome activation while promoting macrophage cell death. In addition, the condition media from cultures of ARPE-19 monolayers wounded with a bisecting scrape was diminished in suppressing phagolysosome activation. This technical report suggests that like primary RPE monolayers, established confluent cultures of ARPE-19 cells produce soluble factors that suppress the activation of macrophages, and can be used to study the molecular mechanisms of retinal immunobiology. In addition, the results further demonstrate the importance of an intact monolayer of RPE cells to modulate immune cell activity within the eye.

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